Chronic in vivo imaging defines age-dependent alterations of neurogenesis in the mouse hippocampus

被引:0
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作者
Yicheng Wu
Sara Bottes
Roberto Fisch
Cinzia Zehnder
John Darby Cole
Gregor-Alexander Pilz
Fritjof Helmchen
Benjamin D. Simons
Sebastian Jessberger
机构
[1] University of Zurich,Laboratory of Neural Plasticity, Faculties of Medicine and Science, Brain Research Institute
[2] University of Zurich,Laboratory of Neural Circuit Dynamics, Faculties of Medicine and Science, Brain Research Institute
[3] University of Cambridge,Wellcome Trust
[4] University of Cambridge,Medical Research Council Stem Cell Institute
[5] University of Cambridge,Wellcome Trust/Cancer Research UK Gurdon Institute
[6] Ludwig Maximilians University,Department of Applied Mathematics and Theoretical Physics, Centre for Mathematical Sciences
来源
Nature Aging | 2023年 / 3卷
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摘要
Neural stem cells (NSCs) generate new neurons throughout life in the mammalian hippocampus1. Advancing age leads to a decline in neurogenesis, which is associated with impaired cognition2,3. The cellular mechanisms causing reduced neurogenesis with advancing age remain largely unknown. We genetically labeled NSCs through conditional recombination driven by the regulatory elements of the stem-cell-expressed gene GLI family zinc finger 1 (Gli1) and used chronic intravital imaging to follow individual NSCs and their daughter cells over months within their hippocampal niche4,5. We show that aging affects multiple steps, from cell cycle entry of quiescent NSCs to determination of the number of surviving cells, ultimately causing reduced clonal output of individual NSCs. Thus, we here define the developmental stages that may be targeted to enhance neurogenesis with the aim of maintaining hippocampal plasticity with advancing age.
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页码:380 / 390
页数:10
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